Biological Signal Detection for Protein Function Prediction. Investigators: Yang Dai Prime Grant Support: NSF. Text File of Protein description. Sequences. Coding Vectors. High-throughput experiments generate new protein sequences with unknown function prediction - PowerPoint PPT Presentation
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Problem Statement and Motivation Key Achievements and Future Goals Technical Approach Biological Signal Detection for Protein Function Prediction Investigators: Yang Dai Prime Grant Support: NSF • High-throughput experiments generate new protein sequences with unknown function prediction • In silico protein function prediction is in need • Protein subcellular localization is a key element in understanding function • Such a prediction can be made based on protein sequences with machine learners • Feature extraction and scalability of learner are keys • Developed highly sophisticated sequence coding methods • Developed an integrated multi-classification system for protein subcellular localization • Developed a preliminary multi-classification system for subnuclear localization • Will incorporate various knowledge from other databases into the current framework • Will design an integrative system for protein function prediction based on information of protein localizations, gene expression, and protein-protein interactions • Use Fast Fourier Transform to capture long range correlation in protein sequence • Design a class of new kernels to capture subtle similarity between sequences • Use domains and motifs of proteins as coding vectors • Use multi-classification system based on deterministic machine learning approach, such as support vector machine • Use Bayesian probabilistic model Sequences specific subcellular and subnuclear localization MASVQLY ... …HKEPGV Machine Learner Text File of Protein descripti on Codin g Vecto rs
Transcript
Problem Statement and Motivation
Key Achievements and Future GoalsTechnical Approach
Biological Signal Detection for Protein Function PredictionInvestigators: Yang Dai
Prime Grant Support: NSF
• High-throughput experiments generate new protein sequences with unknown function prediction
• In silico protein function prediction is in need
• Protein subcellular localization is a key element in understanding function
• Such a prediction can be made based on protein sequences with machine learners
• Feature extraction and scalability of learner are keys
• Developed highly sophisticated sequence coding methods• Developed an integrated multi-classification system for protein
subcellular localization• Developed a preliminary multi-classification system for subnuclear
localization • Will incorporate various knowledge from other databases into the
current framework• Will design an integrative system for protein function prediction based
on information of protein localizations, gene expression, and protein-protein interactions
• Use Fast Fourier Transform to capture long range correlation in protein sequence
• Design a class of new kernels to capture subtle similarity between sequences
• Use domains and motifs of proteins as coding vectors
• Use multi-classification system based on deterministic machine learning approach, such as support vector machine
• Use Bayesian probabilistic model
Sequences
specific subcellular and subnuclear localization
MASVQLY ... …HKEPGV
Machine Learner
Text File of Protein description
Coding Vectors
Problem Statement and Motivation
Key Achievements and Future GoalsTechnical Approach
Computational Protein Topographics for Health Improvement Jie Liang, Ph.D. Bioengineering
Prime Grant Support: National Science Foundation Career Award, National Institutes of Health R01, Office of Naval Research, and the Whitaker Foundation
• The structure of proteins provide rich information about how cells work. With the success of structural genomics, soon we will have all human proteins mapped to structures.
• However, we need to develop computational tools to extract information from these structures to understand how cell works and how new diseases can be treated.
• Therefore, the development of computational tools for surface matching and for function prediction will open the door for many new development for health improvement.
• We have developed a web server CASTP (cast.engr.uic.edu) that identify and measures protein surfaces. It has been used by thousands of scientists world wide.
• We have built a protein surface library for >10,000 proteins, and have developed models to characterize cross reactivities of enzymes.
• We also developed methods for designing phage library for discovery of peptide drugs.
• We have developed methods for predicting structures of beta-barrel membrane proteins.
• Future: Understand how protein fold and assemble, and designing method for engineering better proteins and drugs.
• We use geometric models and fast algorithm to characterize surface properties of over thirty protein structures.
• We develop evolutionary models to understand how proteins overall evolve to acquire different functions using different combination of surface textures.
• Efficient search methods and statistical models allow us to identify very similar surfaces on totally different proteins
• Probablistc models and sampling techniques help us to understand how protein works to perform their functions.
Protein surface matching
Evolution of function
Problem Statement and Motivation
Key Achievements and Future GoalsTechnical Approach
Structural Bioinformatics Study of Protein Interaction NetworkInvestigators: Hui Lu, Bioengineering
Prime Grant Support: NIH, DOL
• Protein interacts with other biomolecules to perform a function: DNA/RNA, ligands, drugs, membranes, and other proteins.
• A high accuracy prediction of the protein interaction network will provide a global understanding of gene regulation, protein function annotation, and the signaling process.
• The understanding and computation of protein-ligand binding have direct impact on drug design.
• Developed the DNA binding protein and binding site prediction protocols that have the best accuracy available.
• Developed transcription factor binding site prediction.• Developed the only protocol that predicts the protein membrane
binding behavior. • Will work on drug design based on structural binding. • Will work on the signaling protein binding mechanism.• Will build complete protein-DNA interaction prediction package and a
Web server.
• Data mining protein structures
• Molecular Dynamics and Monte Carlo simulations
• Machine learning
• Phylogenetic analysis of interaction networks
• Gene expression data analysis using clustering
• Binding affinity calculation using statistical physics
Protein-DNA complex: gene regulation DNA repair cancer treatment drug design gene therapy
Problem Statement and Motivation
Key Achievements and Future GoalsTechnical Approach
Uncovering the mechanism of reversible membrane bindingInvestigators: Hui Lu, Ph.D., Bioengineering
Primary Grant Support: Chicago Biomedical Consortium, NIH
• To efficiently function, cells need to respond properly to external physical and physical and chemical signals in their environment.
• Identifying disease states and designing drugs require a detailed understanding of the internal signaling networks that are activated in responses to external stimuli.
• In the center of these process is a particular group of protein that translocate to the cell membrane upon external activation.
• Developed highly accurate prediction protocols for identifying novel cases of membrane binding proteins, based on properties calculated from molecular surface of the protein structure.
• Determining membrane binding of properties of C2 domains in response to changes in ion placements and membrane lipid composition.
• Goal: To model the network dynamics to understand how changes in membrane binding properties of certain domains changes the efficiency of signal transduction in the cell.
• Combine machine learning techniques with characterization of the protein surface to identify unknown membrane binding proteins.
• Atomic scale molecular dynamics simulation of the interactions between proteins and membranes
• Mathematical modeling is used for studying the spatial and dynamic evolution of the signal transduction networks within the cell when changes in the external environment occurs.
Problem Statement and Motivation
Key Achievements and Future GoalsTechnical Approach
Machine Learning and Datamining in Biomedical InformaticsInvestigators: Hui Lu, Ph.D., Robert Ezra Langlois, Ph.D.,Bioengineering;
Grant Support: NIH, Bioinformatics online
• Massive amount of biomedical data are available from high-throughput measurement, such as genome sequence, proteomics, biological pathway, networks, and disease data.
• Data processing become the bottleneck of biological discovery and medical analysis
• Problem: Protein function prediction, protein functional sites prediction, protein interaction prediction, disease network prediction, biomarker discovery.
• Developed machine learning algorithms for protein-DNA, protein-membrane, protein structure prediction, disease causing SNP prediction, mass-spec data processing, DNA methylation prediction.
• Developed an open-source machine learning software MALIBU
• Goal: Biological network analysis and prediction.
• Formulate the problem in classification problem
• Derive features to represent biological objects
• Develop various classification algorithms
• Develop multiple-instance boosting algorithms
Problem Statement and Motivation
Key Achievements and Future GoalsTechnical Approach
